CD95配体表达调控:免疫调控的关键因素?

Behring Institute Mitteilungen Pub Date : 1996-10-01
T Brunner, N J Yoo, T S Griffith, T A Ferguson, D R Green
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引用次数: 0

摘要

活化T细胞的外周缺失在调节免疫应答的程度方面具有重要作用。经T细胞受体再刺激后,先前受刺激的细胞已被证明死于激活诱导的细胞死亡。最近的研究表明,这一过程是由CD95 (Fas/APO-1)/CD95配体相互作用介导的,从而诱导T细胞凋亡。CD95配体(CD95- l)在未激活的T细胞上不存在,但在刺激下很容易表达。在这里,我们讨论了CD95-L表达是由T细胞受体介导的信号诱导的,并在不同水平上受到调节的证据。不同的激活诱导细胞死亡抑制剂已被发现直接或间接作用于导致CD95-L表达的信号转导途径。CD95-L似乎不仅在T细胞活化后被诱导,而且在许多非淋巴组织中也被发现组成性表达。这表明CD95-L不仅在激活诱导的T细胞死亡中起关键作用,而且可能具有其他功能。其中一个功能是维持免疫特权,保护一些组织免受潜在的破坏性免疫反应。因此,CD95在淋巴细胞和非淋巴细胞中的表达调控似乎是免疫调控的关键因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Regulation of CD95 ligand expression: a key element in immune regulation?

Peripheral deletion of activated T cells has an important function in the regulation of the extent of an immune response. Upon restimulation through the T cell receptor previously stimulated cells have been shown to die by activation-induced cell death. Recent data indicate that this process is mediated by a CD95 (Fas/APO-1)/CD95 ligand interaction which induces apoptosis of the T cell. CD95 ligand (CD95-L) is absent on unactivated T cells but is readily expressed upon stimulation. Here we discuss evidence that CD95-L expression is induced by T cell receptor-mediated signals and is regulated at different levels. Different inhibitors of activation-induced cell death have been found to directly or indirectly act on the signal transduction pathway leading to CD95-L expression. CD95-L seems not only to be induced in T cells after activation but is also found constitutively expressed in many non-lymphoid tissues. This indicates that CD95-L is not only critically involved in activation-induced T cell death, but may have other functions as well. One such function is in the maintenance of immunological privilege, the protection of some tissues from potentially destructive immune responses. Thus, the regulation of CD95 expression in lymphoid and non-lymphoid cells appears to represent a key element in immune regulation.

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